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在单个多隔室生物反应器中模拟 CHO 大规模效应:一种获得放大行为的新方法。

Mimicking CHO large-scale effects in the single multicompartment bioreactor: A new approach to access scale-up behavior.

机构信息

Institute of Biochemical Engineering, University of Stuttgart, Stuttgart, Germany.

Institute of Multiphase Flows, Hamburg University of Technology, Hamburg, Germany.

出版信息

Biotechnol Bioeng. 2024 Apr;121(4):1244-1256. doi: 10.1002/bit.28647. Epub 2024 Jan 8.

DOI:10.1002/bit.28647
PMID:38192095
Abstract

During the scale-up of biopharmaceutical production processes, insufficiently predictable performance losses may occur alongside gradients and heterogeneities. To overcome such performance losses, tools are required to explain, predict, and ultimately prohibit inconsistencies between laboratory and commercial scale. In this work, we performed CHO fed-batch cultivations in the single multicompartment bioreactor (SMCB), a new scale-down reactor system that offers new access to study large-scale heterogeneities in mammalian cell cultures. At volumetric power inputs of 20.4-1.5 W m, large-scale characteristics like long mixing times and dissolved oxygen (DO) heterogeneities were mimicked in the SMCB. Compared to a reference bioreactor (REFB) set-up, the conditions in the SMCB provoked an increase in lactate accumulation of up to 87%, an increased glucose uptake, and reduced viable cell concentrations in the stationary phase. All are characteristic for large-scale performance. The unique possibility to distinguish between the effects of changing power inputs and observed heterogeneities provided new insights into the potential reasons for altered product quality attributes. Apparently, the degree of galactosylation in the evaluated glycan patterns changed primarily due to the different power inputs rather than the provoked heterogeneities. The SMCB system could serve as a potent tool to provide new insights into scale-up behavior and to predict cell line-specific drawbacks at an early stage of process development.

摘要

在生物制药生产工艺的放大过程中,除了梯度和异质性之外,性能损失可能也无法预测。为了克服这些性能损失,需要有工具来解释、预测并最终防止实验室规模和商业规模之间的不一致。在这项工作中,我们在单多室生物反应器(SMCB)中进行了 CHO 分批补料培养,这是一种新的缩小规模的反应器系统,为研究哺乳动物细胞培养中的大规模异质性提供了新的途径。在体积功率输入为 20.4-1.5 W m 时,SMCB 模拟了大规模特征,如较长的混合时间和溶解氧(DO)异质性。与参考生物反应器(REFB)相比,SMCB 中的条件会导致乳酸积累增加高达 87%、葡萄糖摄取增加以及在静止期活细胞浓度降低,所有这些都是大规模性能的特征。能够区分改变功率输入和观察到的异质性的独特可能性,为改变产品质量属性的潜在原因提供了新的见解。显然,在评估的聚糖模式中,半乳糖基化程度的变化主要是由于不同的功率输入,而不是引发的异质性。SMCB 系统可以作为一种有力的工具,在工艺开发的早期阶段提供对放大行为的新见解,并预测细胞系特异性的缺点。

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